Genetic variation in T-box binding element functionally affects SCN5A/SCN10A enhancer

Malou van den Boogaard; L. Y. Elaine Wong; Federico Tessadori; Martijn L. Bakker; Lisa K. Dreizehnter; Vincent Wakker; Connie R. Bezzina; Peter A. C. 't Hoen; Jeroen Bakkers; Phil Barnett; Vincent M. Christoffels

doi:https://doi.org/10.1172/JCI62613

Genetic variation in T-box binding element functionally affects SCN5A/SCN10A enhancer

Malou van den Boogaard, L. Y. Elaine Wong, Federico Tessadori, Martijn L. Bakker, Lisa K. Dreizehnter, Vincent Wakker, Connie R. Bezzina, Peter A. C. 't Hoen, Jeroen Bakkers, Phil Barnett, Vincent M. Christoffels

Research output: Contribution to journal › Article › Academic › peer-review

154 Citations (Scopus)

Abstract

The contraction pattern of the heart relies on the activation and conduction of the electrical impulse. Perturbations of cardiac conduction have been associated with congenital and acquired arrhythmias as well as cardiac arrest. The pattern of conduction depends on the regulation of heterogeneous gene expression by key transcription factors and transcriptional enhancers. Here, we assessed the genome-wide occupation of conduction system-regulating transcription factors TBX3, NKX2-5, and GATA4 and of enhancer-associated coactivator p300 in the mouse heart, uncovering cardiac enhancers throughout the genome. Many of the enhancers colocalized with ion channel genes repressed by TBX3, including the clustered sodium channel genes Scn5a, essential for cardiac function, and Scn10a. We identified 2 enhancers in the Scn5a/Scn10a locus, which were regulated by TBX3 and its family member and activator, TBX5, and are functionally conserved in humans. We also provided evidence that a SNP in the SCN10A enhancer associated with alterations in cardiac conduction patterns in humans disrupts TBX3/TBX5 binding and reduces the cardiac activity of the enhancer in vivo. Thus, the identification of key regulatory elements for cardiac conduction helps to explain how genetic variants in noncoding regulatory DNA sequences influence the regulation of cardiac conduction and the predisposition for cardiac arrhythmias

Original language	English
Pages (from-to)	2519-2530
Journal	Journal of clinical investigation
Volume	122
Issue number	7
DOIs	https://doi.org/10.1172/JCI62613
Publication status	Published - 2012

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https://doi.org/10.1172/JCI62613

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@article{24242f549d9f470b9409d081db79e551,

title = "Genetic variation in T-box binding element functionally affects SCN5A/SCN10A enhancer",

abstract = "The contraction pattern of the heart relies on the activation and conduction of the electrical impulse. Perturbations of cardiac conduction have been associated with congenital and acquired arrhythmias as well as cardiac arrest. The pattern of conduction depends on the regulation of heterogeneous gene expression by key transcription factors and transcriptional enhancers. Here, we assessed the genome-wide occupation of conduction system-regulating transcription factors TBX3, NKX2-5, and GATA4 and of enhancer-associated coactivator p300 in the mouse heart, uncovering cardiac enhancers throughout the genome. Many of the enhancers colocalized with ion channel genes repressed by TBX3, including the clustered sodium channel genes Scn5a, essential for cardiac function, and Scn10a. We identified 2 enhancers in the Scn5a/Scn10a locus, which were regulated by TBX3 and its family member and activator, TBX5, and are functionally conserved in humans. We also provided evidence that a SNP in the SCN10A enhancer associated with alterations in cardiac conduction patterns in humans disrupts TBX3/TBX5 binding and reduces the cardiac activity of the enhancer in vivo. Thus, the identification of key regulatory elements for cardiac conduction helps to explain how genetic variants in noncoding regulatory DNA sequences influence the regulation of cardiac conduction and the predisposition for cardiac arrhythmias",

author = "{van den Boogaard}, Malou and Wong, {L. Y. Elaine} and Federico Tessadori and Bakker, {Martijn L.} and Dreizehnter, {Lisa K.} and Vincent Wakker and Bezzina, {Connie R.} and {'t Hoen}, {Peter A. C.} and Jeroen Bakkers and Phil Barnett and Christoffels, {Vincent M.}",

year = "2012",

doi = "https://doi.org/10.1172/JCI62613",

language = "English",

volume = "122",

pages = "2519--2530",

journal = "Journal of clinical investigation",

issn = "0021-9738",

publisher = "The American Society for Clinical Investigation",

number = "7",

}

TY - JOUR

T1 - Genetic variation in T-box binding element functionally affects SCN5A/SCN10A enhancer

AU - van den Boogaard, Malou

AU - Wong, L. Y. Elaine

AU - Tessadori, Federico

AU - Bakker, Martijn L.

AU - Dreizehnter, Lisa K.

AU - Wakker, Vincent

AU - Bezzina, Connie R.

AU - 't Hoen, Peter A. C.

AU - Bakkers, Jeroen

AU - Barnett, Phil

AU - Christoffels, Vincent M.

PY - 2012

Y1 - 2012

N2 - The contraction pattern of the heart relies on the activation and conduction of the electrical impulse. Perturbations of cardiac conduction have been associated with congenital and acquired arrhythmias as well as cardiac arrest. The pattern of conduction depends on the regulation of heterogeneous gene expression by key transcription factors and transcriptional enhancers. Here, we assessed the genome-wide occupation of conduction system-regulating transcription factors TBX3, NKX2-5, and GATA4 and of enhancer-associated coactivator p300 in the mouse heart, uncovering cardiac enhancers throughout the genome. Many of the enhancers colocalized with ion channel genes repressed by TBX3, including the clustered sodium channel genes Scn5a, essential for cardiac function, and Scn10a. We identified 2 enhancers in the Scn5a/Scn10a locus, which were regulated by TBX3 and its family member and activator, TBX5, and are functionally conserved in humans. We also provided evidence that a SNP in the SCN10A enhancer associated with alterations in cardiac conduction patterns in humans disrupts TBX3/TBX5 binding and reduces the cardiac activity of the enhancer in vivo. Thus, the identification of key regulatory elements for cardiac conduction helps to explain how genetic variants in noncoding regulatory DNA sequences influence the regulation of cardiac conduction and the predisposition for cardiac arrhythmias

AB - The contraction pattern of the heart relies on the activation and conduction of the electrical impulse. Perturbations of cardiac conduction have been associated with congenital and acquired arrhythmias as well as cardiac arrest. The pattern of conduction depends on the regulation of heterogeneous gene expression by key transcription factors and transcriptional enhancers. Here, we assessed the genome-wide occupation of conduction system-regulating transcription factors TBX3, NKX2-5, and GATA4 and of enhancer-associated coactivator p300 in the mouse heart, uncovering cardiac enhancers throughout the genome. Many of the enhancers colocalized with ion channel genes repressed by TBX3, including the clustered sodium channel genes Scn5a, essential for cardiac function, and Scn10a. We identified 2 enhancers in the Scn5a/Scn10a locus, which were regulated by TBX3 and its family member and activator, TBX5, and are functionally conserved in humans. We also provided evidence that a SNP in the SCN10A enhancer associated with alterations in cardiac conduction patterns in humans disrupts TBX3/TBX5 binding and reduces the cardiac activity of the enhancer in vivo. Thus, the identification of key regulatory elements for cardiac conduction helps to explain how genetic variants in noncoding regulatory DNA sequences influence the regulation of cardiac conduction and the predisposition for cardiac arrhythmias

U2 - https://doi.org/10.1172/JCI62613

DO - https://doi.org/10.1172/JCI62613

M3 - Article

C2 - 22706305

SN - 0021-9738

VL - 122

SP - 2519

EP - 2530

JO - Journal of clinical investigation

JF - Journal of clinical investigation

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